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蛋白质超分子结构:从自组装到纳米疫苗设计

Protein Supramolecular Structures: From Self-Assembly to Nanovaccine Design.

作者信息

Zottig Ximena, Côté-Cyr Mélanie, Arpin Dominic, Archambault Denis, Bourgault Steve

机构信息

Department of Chemistry, Université du Québec à Montréal, Montreal, H2L 2C4, Canada.

The Quebec Network for Research on Protein Function, Engineering and Applications, PROTEO, Quebec, G1V 0A6, Canada.

出版信息

Nanomaterials (Basel). 2020 May 25;10(5):1008. doi: 10.3390/nano10051008.

Abstract

Life-inspired protein supramolecular assemblies have recently attracted considerable attention for the development of next-generation vaccines to fight against infectious diseases, as well as autoimmune diseases and cancer. Protein self-assembly enables atomic scale precision over the final architecture, with a remarkable diversity of structures and functionalities. Self-assembling protein nanovaccines are associated with numerous advantages, including biocompatibility, stability, molecular specificity and multivalency. Owing to their nanoscale size, proteinaceous nature, symmetrical organization and repetitive antigen display, protein assemblies closely mimic most invading pathogens, serving as danger signals for the immune system. Elucidating how the structural and physicochemical properties of the assemblies modulate the potency and the polarization of the immune responses is critical for bottom-up design of vaccines. In this context, this review briefly covers the fundamentals of supramolecular interactions involved in protein self-assembly and presents the strategies to design and functionalize these assemblies. Examples of advanced nanovaccines are presented, and properties of protein supramolecular structures enabling modulation of the immune responses are discussed. Combining the understanding of the self-assembly process at the molecular level with knowledge regarding the activation of the innate and adaptive immune responses will support the design of safe and effective nanovaccines.

摘要

受生命启发的蛋白质超分子组装体最近在开发用于对抗传染病、自身免疫性疾病和癌症的下一代疫苗方面引起了广泛关注。蛋白质自组装能够在最终结构上实现原子尺度的精确性,具有显著多样的结构和功能。自组装蛋白质纳米疫苗具有许多优点,包括生物相容性、稳定性、分子特异性和多价性。由于其纳米级尺寸、蛋白质性质、对称组织和重复抗原展示,蛋白质组装体紧密模拟大多数入侵病原体,充当免疫系统的危险信号。阐明组装体的结构和物理化学性质如何调节免疫反应的效力和极化对于疫苗的自下而上设计至关重要。在此背景下,本综述简要介绍了蛋白质自组装中涉及的超分子相互作用的基本原理,并介绍了设计这些组装体并使其功能化的策略。展示了先进纳米疫苗的实例,并讨论了能够调节免疫反应的蛋白质超分子结构的性质。将分子水平上对自组装过程的理解与关于先天免疫和适应性免疫反应激活的知识相结合,将有助于设计安全有效的纳米疫苗。

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